PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.

A variety of ubiquitinated protein-containing cytoplasmic structures has been reported, from aggresomes to aggresome-like induced structures/sequestosomes or particle-rich cytoplasmic structures (PaCSs) that we recently observed in some human diseases. Nevertheless, the morphological and cytochemica...

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Main Authors: Patrizia Sommi, Vittorio Necchi, Agostina Vitali, Daniela Montagna, Ada De Luigi, Mario Salmona, Vittorio Ricci, Enrico Solcia
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3866174?pdf=render
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spelling doaj-b351f285a344414297f0c014847e35392020-11-24T21:50:06ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01812e8256010.1371/journal.pone.0082560PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.Patrizia SommiVittorio NecchiAgostina VitaliDaniela MontagnaAda De LuigiMario SalmonaVittorio RicciEnrico SolciaA variety of ubiquitinated protein-containing cytoplasmic structures has been reported, from aggresomes to aggresome-like induced structures/sequestosomes or particle-rich cytoplasmic structures (PaCSs) that we recently observed in some human diseases. Nevertheless, the morphological and cytochemical patterns of the different structures remain largely unknown thus jeopardizing their univocal identification. Here, we show that PaCSs resulted from proteasome and polyubiquitinated protein accumulation into well-demarcated, membrane-free, cytoskeleton-poor areas enriched in glycogen and glycosaminoglycans. A major requirement for PaCS detection by either electron or confocal microscopy was the addition of osmium to aldehyde fixatives. However, by analyzing living cells, we found that proteasome chymotrypsin-like activity concentrated in well-defined cytoplasmic structures identified as PaCSs by ultrastructural morphology and immunocytochemistry of the same cells. PaCSs differed ultrastructurally and cytochemically from sequestosomes which may coexist with PaCSs. In human dendritic or natural killer cells, PaCSs were induced in vitro by cytokines/trophic factors during differentiation/activation from blood progenitors. Our results provide evidence that PaCS is indeed a novel distinctive cytoplasmic structure which may play a critical role in the ubiquitin-proteasome system response to immune, infectious or proneoplastic stimuli.http://europepmc.org/articles/PMC3866174?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Patrizia Sommi
Vittorio Necchi
Agostina Vitali
Daniela Montagna
Ada De Luigi
Mario Salmona
Vittorio Ricci
Enrico Solcia
spellingShingle Patrizia Sommi
Vittorio Necchi
Agostina Vitali
Daniela Montagna
Ada De Luigi
Mario Salmona
Vittorio Ricci
Enrico Solcia
PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.
PLoS ONE
author_facet Patrizia Sommi
Vittorio Necchi
Agostina Vitali
Daniela Montagna
Ada De Luigi
Mario Salmona
Vittorio Ricci
Enrico Solcia
author_sort Patrizia Sommi
title PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.
title_short PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.
title_full PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.
title_fullStr PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.
title_full_unstemmed PaCS is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.
title_sort pacs is a novel cytoplasmic structure containing functional proteasome and inducible by cytokines/trophic factors.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description A variety of ubiquitinated protein-containing cytoplasmic structures has been reported, from aggresomes to aggresome-like induced structures/sequestosomes or particle-rich cytoplasmic structures (PaCSs) that we recently observed in some human diseases. Nevertheless, the morphological and cytochemical patterns of the different structures remain largely unknown thus jeopardizing their univocal identification. Here, we show that PaCSs resulted from proteasome and polyubiquitinated protein accumulation into well-demarcated, membrane-free, cytoskeleton-poor areas enriched in glycogen and glycosaminoglycans. A major requirement for PaCS detection by either electron or confocal microscopy was the addition of osmium to aldehyde fixatives. However, by analyzing living cells, we found that proteasome chymotrypsin-like activity concentrated in well-defined cytoplasmic structures identified as PaCSs by ultrastructural morphology and immunocytochemistry of the same cells. PaCSs differed ultrastructurally and cytochemically from sequestosomes which may coexist with PaCSs. In human dendritic or natural killer cells, PaCSs were induced in vitro by cytokines/trophic factors during differentiation/activation from blood progenitors. Our results provide evidence that PaCS is indeed a novel distinctive cytoplasmic structure which may play a critical role in the ubiquitin-proteasome system response to immune, infectious or proneoplastic stimuli.
url http://europepmc.org/articles/PMC3866174?pdf=render
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